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BPIFA2作为一种新型早期生物标志物用于识别辐射暴露后的致死性辐射损伤。

BPIFA2 as a Novel Early Biomarker to Identify Fatal Radiation Injury After Radiation Exposure.

作者信息

He Lexin, Zhou Shixiang, Li Weihong, Wang Qi, Qi Zhenhua, Zhou Pingkun, Wang Zhidong, Chen Jing, Li Yaqiong, Lin Zhongwu

机构信息

College of Life Sciences, North China University of Science and Technology, Tangshan, China.

Department of Radiobiology, Beijing Key Laboratory for Radiobiology, Beijing Institute of Radiation Medicine, Beijing, China.

出版信息

Dose Response. 2022 Apr 11;20(1):15593258221086478. doi: 10.1177/15593258221086478. eCollection 2022 Jan-Mar.

Abstract

BACKGROUND

Current dosimeters cannot cope with the two tasks of medical rescue in the early stage of nuclear accident, the accurate determination of radiation exposure and the identification of patients with fatal radiation injury. As radiation can cause alterations in serum components, it is feasible to develop biomarkers for radiation injury from serum. This study aims to investigate whether serum BPIFA2 could be used as a potential biomarker of predicting fatal radiation injury in the early stage after nuclear accident.

METHODS

A rabbit anti-mouse BPIFA2 polyclonal antibody was prepared to detect the expression of BPIFA2. C57BL/6J female mice were exposed to total body radiation (TBI) at different dose and Partial body radiation (PBI) at lethal dose to detect the dynamic changes of BPIFA2 in serum at different time points after irradiation by Western blot assay.

RESULTS

BPIFA2 in mice serum were significantly increased at 1-12 h post-irradiation at .5-10 Gy, and increased again significantly at 3 d after 10 Gy irradiation with associated with mortality closely. It also increased rapidly after PBI and was closely related to injury degree, regardless whether the salivary glands were irradiated.

CONCLUSIONS

The increase of serum BPIFA2 is a novel early biomarker not only for identifying radiation exposure, but also for fatal radiation injury playing a vital role in rational use of medical resources, and greater efficiency of medical treatment to minimize casualties.

摘要

背景

目前的剂量计无法应对核事故早期医学救援的两项任务,即准确测定辐射暴露以及识别致命性辐射损伤患者。由于辐射可导致血清成分改变,因此从血清中开发辐射损伤生物标志物是可行的。本研究旨在探讨血清BPIFA2是否可作为预测核事故后早期致命性辐射损伤的潜在生物标志物。

方法

制备兔抗小鼠BPIFA2多克隆抗体以检测BPIFA2的表达。将C57BL/6J雌性小鼠暴露于不同剂量的全身辐射(TBI)和致死剂量的局部身体辐射(PBI),通过蛋白质免疫印迹法检测照射后不同时间点血清中BPIFA2的动态变化。

结果

在0.5 - 10 Gy照射后1 - 12小时,小鼠血清中的BPIFA2显著增加,在10 Gy照射后3天再次显著增加,且与死亡率密切相关。在局部身体辐射后它也迅速增加,并且与损伤程度密切相关,无论唾液腺是否受到照射。

结论

血清BPIFA2的升高是一种新的早期生物标志物,不仅可用于识别辐射暴露,还可用于致命性辐射损伤,在合理利用医疗资源以及提高医疗效率以尽量减少伤亡方面发挥着至关重要的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/417f/9006374/60ea641f36d2/10.1177_15593258221086478-fig1.jpg

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